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首页> 外文期刊>Psychopharmacology >Effects of mGluR1 antagonism in the dorsal hippocampus on drug context-induced reinstatement of cocaine-seeking behavior in rats.
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Effects of mGluR1 antagonism in the dorsal hippocampus on drug context-induced reinstatement of cocaine-seeking behavior in rats.

机译:背海马mGluR1拮抗作用对药物环境诱导的大鼠可卡因寻找行为的恢复作用。

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RATIONALE: The functional integrity of the dorsal hippocampus (DH) is necessary for drug context-induced reinstatement of cocaine seeking. However, the neuropharmacological mechanisms of this phenomenon are poorly understood. OBJECTIVES: Given the known significance of group I metabotropic glutamate receptors (mGluRs), including the mGluR1 subtype, in drug-induced behaviors, the present study was designed to evaluate the contribution of mGluR1s in the DH to drug context-induced reinstatement of extinguished cocaine-seeking behavior. METHODS: Sprague-Dawley rats were trained to lever press for unsignaled cocaine infusions in a distinct environmental context (cocaine-paired context) followed by extinction training in a distinctly different environmental context (extinction context). Using a counterbalanced partial within-subjects testing design, rats were re-exposed to the cocaine-paired context or the extinction context while cocaine-seeking behavior (nonreinforced active lever pressing) was assessed. Prior to each test session, rats received bilateral microinfusions of the highly potent mGluR1-selective antagonist JNJ16259685 (0.6, 30, or 120 pg/0.5 microl per hemisphere) or vehicle into the DH or the overlying somatosensory cortex trunk region (SStr; anatomical control). RESULTS: Intra-DH, but not intra-SStr, JNJ16259685 infusions dose dependently attenuated drug context-induced reinstatement of cocaine seeking relative to vehicle treatment, without attenuating instrumental behavior in the extinction context, general motor activity, or food-reinforced instrumental behavior in control experiments. CONCLUSIONS: Stimulation of mGluR1s in the DH is necessary for incentive motivational and/or memory processes that contribute to drug context-induced cocaine-seeking behavior. These findings indicate that the mGluR1 is an interesting target from an addiction treatment perspective.
机译:理由:药物引起的可卡因恢复可能需要海马背侧(DH)的功能完整。但是,这种现象的神经药理机制了解甚少。目的:鉴于已知的第一类代谢型谷氨酸受体(mGluRs),包括mGluR1亚型,在药物诱导的行为中,本研究旨在评估DH中的mGluR1对药物环境诱导的可卡因恢复的作用寻求行为。方法:对Sprague-Dawley大鼠进行训练,使其在不同的环境情况下(可卡因配对的情况下)按压力进行无信号的可卡因输注,然后在截然不同的环境情况下(灭绝的情况下)进行灭绝训练。使用平衡的部分受试者内部测试设计,将大鼠重新暴露于可卡因配对的环境或灭绝的环境中,同时评估可卡因的寻找行为(未增强的主动杠杆按压)。在每次测试之前,大鼠均向DH或上方的躯体感觉皮层躯干区域(SStr;解剖学对照)中接受了高效mGluR1选择性拮抗剂JNJ16259685(每半球0.6、30或120 pg / 0.5微升)或运载体的双侧微输注。 )。结果:相对于媒介物治疗,DH内,而不是SStr内,JNJ16259685输注剂量依赖性地减弱了药物引起的可卡因恢复,而不减弱灭绝环境下的器械行为,一般运动活动或食物强化的器械行为对照实验。结论:DH中的mGluR1的刺激对于激励性动机和/或记忆过程是必要的,这些过程有助于药物引起的可卡因寻求行为。这些发现表明,从成瘾治疗的角度来看,mGluR1是一个有趣的靶标。

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